Phenotypes associated with this allele

• Allele Symbol: Thbd^tm1Wlr
• Allele Name: targeted mutation 1, Harmut Weiler
• Allele ID: MGI:2158812
• Summary: 2 genotypes

Jump to	Allelic Composition	Genetic Background	Genotype ID
hm1	Thbd^tm1Wlr/Thbd^tm1Wlr	B6.129S2-Thbd^tm1Wlr	MGI:3844993
ht2	Thbd^tm1Wlr/Thbd^tm2Rdr	involves: 129S2/SvPas * C57BL/6	MGI:3844986

Genotype
MGI:3844993

hm1

• Allelic Composition: Thbd^tm1Wlr/Thbd^tm1Wlr
• Genetic Background: B6.129S2-Thbd^tm1Wlr

• ♀: phenotype observed in females
• ♂: phenotype observed in males
• N: normal phenotype

mortality/aging

increased susceptibility to induced morbidity/mortality ( J:111502 )

• LPS-treated mice exhibit increased mortality compared with similarly treated wild-type mice

homeostasis/metabolism

increased circulating D-dimer level ( J:111502 )

• plasma D-dimer levels are increased compared to in wild-type mice

increased circulating interleukin-1 beta level ( J:111502 )

• LPS-treated mice exhibit increased IL1beta serum levels compared with similarly treated wild-type mice

increased circulating interleukin-6 level ( J:111502 )

• LPS-treated mice exhibit increased IL6 serum levels compared with similarly treated wild-type mice

decreased circulating tumor necrosis factor level ( J:111502 )

• LPS-treated mice exhibit a 2-fold reduction in serum TNFalpha levels compared with similarly treated wild-type mice

abnormal blood coagulation ( J:111502 )

• plasma thrombin-antithrombin (TAT), D-dimer, fibrinopeptide A (FPA), and plasmin-antiplasmin (PAP) are increased compared to in wild-type mice

• however, mice control bleeding normally after an initial period of increased blood loss

increased susceptibility to induced thrombosis ( J:111502 )

• after FeCl3-induced injury mice exhibit accelerated arterial thrombus growth compared with wild-type mice

• following ligation near the carotid bifurcation, mice exhibit more extensive thrombotic lesions with increased neointimal mass over the entire length of the artery, halfway towards the aortic arch, or over the distal third of the ligated vessel compared with similarly treated wild-type mice that develop thrombic lesions within 1 mm of the ligation site

immune system

abnormal spleen morphology ( J:111502 )

• LPS-induced fibrin deposits are more pronounced than in similarly treated wild-type mice

• however, no abnormal fibrin deposits are observed in un-induced mice

increased circulating interleukin-1 beta level ( J:111502 )

• LPS-treated mice exhibit increased IL1beta serum levels compared with similarly treated wild-type mice

increased circulating interleukin-6 level ( J:111502 )

• LPS-treated mice exhibit increased IL6 serum levels compared with similarly treated wild-type mice

decreased circulating tumor necrosis factor level ( J:111502 )

• LPS-treated mice exhibit a 2-fold reduction in serum TNFalpha levels compared with similarly treated wild-type mice

increased susceptibility to endotoxin shock ( J:111502 )

• LPS-treated mice exhibit increased mortality, elevated IL6 and IL1beta serum levels, decreased TNFalpha serum levels, and increased fibrin deposits in the kidney, heart, spleen, and lung compared with similarly treated wild-type mice

hematopoietic system

abnormal spleen morphology ( J:111502 )

• LPS-induced fibrin deposits are more pronounced than in similarly treated wild-type mice

• however, no abnormal fibrin deposits are observed in un-induced mice

cardiovascular system

abnormal heart morphology ( J:111502 )

• LPS-induced fibrin deposits are more pronounced than in similarly treated wild-type mice

• however, no abnormal fibrin deposits are observed in un-induced mice

renal/urinary system

abnormal kidney morphology ( J:111502 )

• LPS-induced fibrin deposits are more pronounced than in similarly treated wild-type mice

respiratory system

abnormal lung morphology ( J:111502 )

• LPS-induced fibrin deposits are more pronounced than in similarly treated wild-type mice

• however, no abnormal fibrin deposits are observed in un-induced mice

Genotype
MGI:3844986

ht2

• Allelic Composition: Thbd^tm1Wlr/Thbd^tm2Rdr
• Genetic Background: involves: 129S2/SvPas * C57BL/6

cardiovascular system

abnormal heart morphology ( J:47676 , J:111502 )

• fibrin deposition is increased 10- to 20-fold compared to in wild-type mice (J:47676)

• fibrin deposition is increased compared to in wild-type mice (J:111502)

immune system

abnormal spleen morphology ( J:47676 , J:111502 )

• fibrin deposition is increased 10- to 20-fold compared to in wild-type mice (J:47676)

• fibrin deposition is increased compared to in wild-type mice (J:111502)

respiratory system

abnormal lung morphology ( J:47676 , J:111502 )

• fibrin deposition is increased 10- to 20-fold compared to in wild-type mice (J:47676)

• fibrin deposition is increased compared to in wild-type mice (J:111502)

homeostasis/metabolism

increased circulating D-dimer level ( J:111502 )

• plasma D-dimer levels are increased compared to in wild-type mice

abnormal blood coagulation ( J:111502 )

• plasma thrombin-antithrombin (TAT) and D-dimer are increased compared to in wild-type mice

abnormal lung thrombosis ( J:47676 )

• under hypoxic conditions, mice exhibit a 10-fold increase in fibrin depositions in the lung compared with a 4- to 5-fold increase in similarly treated wild-type mice

increased susceptibility to induced thrombosis ( J:111502 )

• after FeCl3-induced injury mice exhibit accelerated arterial thrombus growth compared with wild-type mice

hematopoietic system

abnormal spleen morphology ( J:47676 , J:111502 )

• fibrin deposition is increased 10- to 20-fold compared to in wild-type mice (J:47676)

• fibrin deposition is increased compared to in wild-type mice (J:111502)